While misdiagnosis of restless legs syndrome remains common, the Food and Drug Administration has increased the agents available to treat this movement disorder by approving the dopamine agonist pramipexole for moderate to severe cases.
Pramipexole is the second drug and the second dopamine agonist to be approved for this condition. The first was ropinirole (Requip), another dopamine agonist approved last year for restless legs syndrome (RLS), which affects as many as 3% of the population.
Dopamine agonists have been considered first-line treatments for RLS by expert consensus panels before they were approved, according to Dr. John Winkelman, who is medical director of the sleep health center at Brigham and Women's Hospital, and Harvard Medical School in Boston.
Although it will take more time for recognition of RLS to improve, “the good news is that the treatments are so effective and generally so well tolerated, it is very gratifying to treat,” and treatment typically produces a rapid response, Dr. Winkelman said.
In his experience, it is “the unusual patient who does not have some response to one of the dopamine agonists, and you need to go back and reassess the diagnosis” in patients who have no response.
Both pramipexole, marketed as Mirapex by Boehringer Ingelheim, and ropinirole, marketed as Requip, have been available for almost 10 years, since they were approved for Parkinson's disease. (Dr. Winkelman is a consultant to Boehringer Ingelheim and to ropinirole manufacturer GlaxoSmithKline, as well as other companies that manufacture products for insomnia and other sleep disorders.)
Pramipexole was significantly more effective than placebo in four randomized, double-blind, 3− to 12-week studies of about 1,000 patients with moderate to severe RLS, which evaluated the effect of treatment on a scale based on patient-reported symptoms and a Clinical Global Impressions scale.
Dr. Winkelman was the lead author of one study of 344 patients, published in September, which found that at 12 weeks, the patients on three fixed doses of pramipexole had significantly greater improvements from baseline than those on placebo in a scale that represented patient rating of symptom severity, which covers different aspects of RLS, such as effects on sleep and next-day functioning.
In addition, 70%–75% of patients on the three doses of pramipexole studied were rated as “very much improved” or “much improved” on a clinician rating scale, compared with 51% of those on placebo, a significant difference (Neurology 2006;67:1034–9). A strong placebo effect was seen on both of these primary end points, which Dr. Winkelman noted was true for disorders in which people are asked how they are doing.
Side effects were generally mild, with no serious adverse events considered drug-related, Dr. Winkelman said. Nausea was the main side effect that was more common in patients on the drug (19% vs. almost 5%) but was mild and transient.
Because this was a forced titration study, in which patients were titrated up to the preassigned dose even if they responded to a lower dose, side effects may have been more common than if the doses were individualized, he said.
Interestingly, a benefit of the low dose of 0.125 mg over placebo was seen at 1 week, he pointed out.
Restless legs syndrome becomes more prevalent as people age, with the typical age of onset in the 40s and 50s. The symptoms and effects of the disorder are not well recognized, he said, noting that RLS substantially interferes with a person's ability to fall asleep and stay asleep, and with their daytime functioning. People with moderate to severe RLS have symptoms “more often than not”–at least three times a week.
The indications section of the revised label for pramipexole lists diagnostic criteria for restless legs syndrome, including an urge to move the legs that is “usually accompanied or caused by uncomfortable and unpleasant leg sensations,” symptoms that begin or worsen during periods of inactivity, such as lying or sitting; and symptoms that are partially or totally relieved by movement such as walking or stretching, for at least as long as the activity continues.
“Why a dopamine agonist works in restless legs syndrome is not entirely clear,” he said. Dopamine is involved in the regulation of movement, and potentially in sensorimotor integration, and RLS is considered a sensorimotor disorder.
The dopamine agonist doses used for RLS are much lower than doses used to treat Parkinson's. The FDA-recommended starting dose is 0.125 mg taken once daily 2–3 hours before bedtime. If necessary, the dose can be increased every 4–7 days to 0.25 mg daily, and if necessary, to 0.5 mg daily after another 4–7 days.